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首页> 外文期刊>International Journal of Radiation Oncology, Biology, Physics >Nuclear expression of human apurinic/apyrimidinic endonuclease (HAP1/Ref-1) in head-and-neck cancer is associated with resistance to chemoradiotherapy and poor outcome.
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Nuclear expression of human apurinic/apyrimidinic endonuclease (HAP1/Ref-1) in head-and-neck cancer is associated with resistance to chemoradiotherapy and poor outcome.

机译:人嘌呤/嘧啶核糖核酸内切酶(HAP1 / Ref-1)在头颈癌中的核表达与对放化疗的抵抗力和不良预后相关。

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摘要

PURPOSE: HAP1/Ref-1 endonuclease is involved in the repair of DNA strand breaks and in the activation of DNA binding of several transcription factors. HAP1 is also a potent activator of wild type p53. It therefore has multiple possible roles in the response of human cancer to radiotherapy and chemotherapy. METHODS AND MATERIALS: The nuclear expression of HAP1 and p53 proteins was studied by immunohistochemistry in paraffin-embedded material from 95 patients with locally advanced squamous cell head-and-neck cancer (HNC) treated with radical radiotherapy (38 cases with induction platinum-based chemotherapy and 57 with concurrent platinum chemoradiotherapy). RESULTS: HAP1 was present in the nuclei of normal epithelium and stromal cells. Loss of HAP1 nuclear expression was frequently noted in cancer cells. Tumors with high HAP1 nuclear expression (% of positive cells > mean; mean = 11%) were of good differentiation (p = 0.06) and presented frequently with advanced nodal disease (p = 0.01). High nuclear HAP1 expression was significantly associated with poor complete response rate (p = 0.00001), shorter local relapse-free interval (p < 0.0001), and poorer survival (p < 0.0008). HAP1 nuclear reactivity was inversely associated with p53 nuclear accumulation (p = 0.003). The inverse correlation between HAP1 expression and prognosis was independent of p53 status. CONCLUSION: HAP1 nuclear expression in HNC is inversely associated with p53 nuclear accumulation and directly related to resistance to chemoradiotherapy and poor survival. Further clinical investigation is required to confirm these findings.
机译:目的:HAP1 / Ref-1核酸内切酶参与DNA链断裂的修复以及几种转录因子的DNA结合的激活。 HAP1还是野生型p53的有效激活剂。因此,它在人类癌症对放射疗法和化学疗法的反应中具有多种可能的作用。方法和材料:采用免疫组织化学方法研究了95例接受局部放疗的局部晚期鳞状细胞头颈癌(HNC)患者的石蜡包埋材料中HAP1和p53蛋白的核表达(38例诱导铂基化疗和57例同时进行铂放化疗。结果:HAP1存在于正常上皮和基质细胞的细胞核中。癌细胞中经常注意到HAP1核表达的丧失。具有高HAP1核表达的肿瘤(阳性细胞百分比>平均;平均= 11%)具有良好的分化能力(p = 0.06),并经常出现晚期淋巴结病(p = 0.01)。 HAP1核高表达与不良反应(p = 0.00001),局部无复发间隔时间较短(p <0.0001)和生存不良(p <0.0008)显着相关。 HAP1核反应性与p53核积累呈负相关(p = 0.003)。 HAP1表达与预后之间的负相关与p53状态无关。结论:HNC中HAP1的核表达与p53的核蓄积呈负相关,与对放化疗的抵抗力和生存不良直接相关。需要进一步的临床研究以证实这些发现。

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